The 10th European Congress on Menopause and Andropause (EMAS 2015), Spain, Madrid, 20-22 May 2015. How to Cite?

Abstract

BACKGROUND: Menopause is a major life stage of women. Premature or early menopause can be associated with several diseases. Age at menopause is a highly heritable trait. Previous genome-wide meta-analysis in European and northern Chinese identified 26 loci underlying age at menopause. In the current study, we aim at validating these loci in 653 Hong Kong southern Chinese women. MATERIALS AND METHODS: This study was performed on 653 women who participated in the Hong Kong Osteoporosis Study, whose age at menopause was available. These women consented to have blood taken and archived for genotyping. DNA was extracted from the buffy coat, and genotyping was performed using Sequenom iPLEX. Age at menopause was recorded using a structured questionnaire. In this study, 60 subjects with early menopause (defined as age at menopause <45 years) were compared to 397 subjects with age at menopause >= 50 years. The associations of 26 single-nucleotide polymorphisms (SNPs), previously reported in Europeans and northern Chinese, with age at menopause (continuous variable) and early menopause (dichotomized variable) were examined using linear regression and logistic regression, respectively. RESULTS: Among those genotyped loci, rs10183486, rs11668344, and rs365132 showed significant replication with age at menopause with an effect size of the minor allele being -0.025 (P=0.036), -0.016 (P=0.019), and 0.009 (P=0.017), respectively. Similarly, these SNPs (rs10183486, rs11668344, and rs365132) were also associated with risk of early menopause with the odds ratio of the minor allele being 2.39 (P=0.047), 1.88 (P=0.029), and 0.711 (P=0.043), respectively. In addition, rs10852344 also showed significant replication with the risk of early menopause with an odds ratio of 0.59 (P=0.029). CONCLUSION: The current study provides independent evidence that rs10183486, rs11668344, rs365132, and possibly rs10852344 are determinants of age at menopause in southern Chinese. The mechanisms of how these associated genes act towards occurrence of menopause warrants further investigation.

The 10th European Congress on Menopause and Andropause (EMAS 2015), Spain, Madrid, 20-22 May 2015.

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dc.identifier.uri

http://hdl.handle.net/10722/209361

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dc.description.abstract

BACKGROUND: Menopause is a major life stage of women. Premature or early menopause can be associated with several diseases. Age at menopause is a highly heritable trait. Previous genome-wide meta-analysis in European and northern Chinese identified 26 loci underlying age at menopause. In the current study, we aim at validating these loci in 653 Hong Kong southern Chinese women. MATERIALS AND METHODS: This study was performed on 653 women who participated in the Hong Kong Osteoporosis Study, whose age at menopause was available. These women consented to have blood taken and archived for genotyping. DNA was extracted from the buffy coat, and genotyping was performed using Sequenom iPLEX. Age at menopause was recorded using a structured questionnaire. In this study, 60 subjects with early menopause (defined as age at menopause <45 years) were compared to 397 subjects with age at menopause >= 50 years. The associations of 26 single-nucleotide polymorphisms (SNPs), previously reported in Europeans and northern Chinese, with age at menopause (continuous variable) and early menopause (dichotomized variable) were examined using linear regression and logistic regression, respectively. RESULTS: Among those genotyped loci, rs10183486, rs11668344, and rs365132 showed significant replication with age at menopause with an effect size of the minor allele being -0.025 (P=0.036), -0.016 (P=0.019), and 0.009 (P=0.017), respectively. Similarly, these SNPs (rs10183486, rs11668344, and rs365132) were also associated with risk of early menopause with the odds ratio of the minor allele being 2.39 (P=0.047), 1.88 (P=0.029), and 0.711 (P=0.043), respectively. In addition, rs10852344 also showed significant replication with the risk of early menopause with an odds ratio of 0.59 (P=0.029). CONCLUSION: The current study provides independent evidence that rs10183486, rs11668344, rs365132, and possibly rs10852344 are determinants of age at menopause in southern Chinese. The mechanisms of how these associated genes act towards occurrence of menopause warrants further investigation.

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dc.language

eng

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dc.relation.ispartof

European Congress on Menopause & Andropause, EMAS 2015

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dc.title

Association of single nucleotide polymorphisms with age at menopause in Hong Kong Chinese women